Title: OrexinHypocretin enhances synaptic strength in VTA dopamine neurons
1Orexin/Hypocretin enhances synaptic strength in
VTA dopamine neurons
- Stephanie Borgland, Ph.D.
- Ernest Gallo Clinic and Research Center, UCSF
2Orexin/Hypocretin and Reward
- Orexin/Hypocretin increases VTA neuron firing
(Korotkova et al., 2003) - Intra-VTA orexin/hypocretin increases dopamine in
the Nucleus Accumbens (Narita et al., 2006) or
PFC (Vittoz and Berridge, 2006) - Orexin/Hypocretin neurons are activated when rats
prefer morphine in a CPP paradigm which is
blocked by intra VTA hypocretin antagonist
(Harris et al., 2005) - CPP for morphine is abolished in
orexin/hypocretin peptide knockout mice (Narita
et al., 2006). - Orexin/hypocretin i.c.v. reinstates cocaine
seeking (Boutrel et al., 2006)
3How does orexin/hypocretin mediate the rewarding
effects of drugs?
- Can ox/hcrt cause synaptic plasticity in
dopamine neurons?
4Why is synaptic plasticity in the VTA important?
- Glutamatergic synaptic plasticity plays a key
role in neural plasticity relevant to addiction - Induction of behavioral sensitization is
dependent on activation of NMDA receptors in the
VTA (Kalivas and Alesdatter, 1993) - Synaptic plasticity of dopamine neurons in the
VTA may play a key role in the reinforcement of
reward.
5Patch Clamp Recording from VTA neurons
NMDA EPSC 40 mV
AMPA EPSC -70 mV
Currents
6OxA/Hcrt1 concentration-dependently increases
NMDAR EPSCs in VTA neurons
n12
7OxA/Hcrt1 does not potentiate AMPA EPSCs in VTA
neurons
n8
8Orexin/Hypocretin Pharmacology
9OxA/Hcrt1 mediated potentiation of NMDAR EPSCs is
inhibited by OX1/hcrt1 receptor antagonist
n8
10LH-hcrt neuron
OXR1
OXA
OXA
OXA
OXA
NMDAR
PLC/PKC
NR1
1
NR2A/?
GLU
NR1/NR2A/?
PFC PPN
AMPA
VTA Neuron
2
NR1
NR2A/?
11OxA/Hcrt1 on AMPAR synaptic transmission
- Activation of NMDARs is an important component
for VTA long term potentiation (LTP) - AMPAR/NMDAR is measure of LTP
12NMDAR activation precedes AMPAR plasticity
OxA/Hcrt1, CRF, cocaine
NMDARs
AMPARs
13NMDAR activation precedes AMPAR plasticity
Stress, cocaine, other drugs of abuse
AMPARs
NMDARs
Time (?)
Does orexin A potentiation of NMDARs facilitate
cocaine-mediated AMPAR plasticity?
14OXR1/Hcrt1R antagonist blocks cocaine induced
potentiation of AMPAR/NMDAR ratio
n4
n4
n5
5 days cocaine or saline /- OXR1 antagonist
n11
15OXR1/Hcrt1R antagonist blocks cocaine induced
potentiation of AMPAR/NMDAR ratio
n11
n5
n4
n4
5 days cocaine or saline /- OXR1 antagonist
16Does OxA/Hcrt1 increase AMPA/NMDA ratio?
Recording
Recording
Slices are incubated with OxA/Hcrt1 for 5 minutes
VTA
3-4 hours
15 minutes
17OxA/Hcrt1 increases AMPAR/NMDAR hours after
application
n8
n8
n8
18OxA/Hcrt1 causes a late phase increase in AMPAR
mediated synaptic transmission
15 min
3-4 hours
control
(7) (6) (7)
19OxA/Hcrt1 causes a late phase increase in AMPAR
mediated synaptic transmission that is NMDAR
dependent
15 min
3-4 hours
control
(7) (6) (7) (7)
20Does OxA/Hcrt1 mediated plasticity of dopamine
neurons have behavioral consequences?
- Activation of NMDARs is an important component
for VTA LTP (Bonci Malenka, 1999) and the
development of cocaine sensitization (Kalivas
Alesdatter, 1993) - Behavioral sensitization is a progressive
increase in locomotor response to the same
cocaine dose. - Since cocaine sensitization is dependent on NMDAR
activation in the VTA, we hypothesized that
OxA/Hcrt1 may have a role in behavioral
sensitization to cocaine.
21OXR1/Hcrt1R antagonist blocks cocaine
sensitization
n13
22Behavioral sensitization is blocked with
intra-VTA injections of OXR1/Hcrt1R antagonist
Cocaine (ip)
Intra-VTA vehicle (12)
Intra-VTA SB334867 (12)
Saline (ip)
Intra-VTA vehicle (8)
Intra-VTA SB334867 (10)
23Hypothesis
Orexin/hypocretin has a profound role in altering
synaptic plasticity in a neural circuit important
for motivation Does orexin/hypocretin signaling
mediate motivated behavior? ie. if
orexin/hypocretin receptors are blocked, will
rats work as much to get cocaine?
24Self-administration Progressive Ratio
0.5 mg/infusion cocaine Paired with tone and light
Progressive ratio
1 2 3 4
Surgery
FR5
FR3
FR1
Naive
Vehicle
Vehicle
SB 334867
25Vehicle treated rats do not reduce pressing for
the duration of the experiment
n8
26OXR1/Hcrt1 antagonist reduces motivation in
progressive ratio test in cocaine
self-administering rats
SB 334867 10 mg/kg
n12
27Cumulative response shows the pattern of presses
for cocaine in vehicle and SB334867 treated rats
RatS5
n12
28Food self administration
n9
29Orexin/Hcrt 1 receptor signaling is not involved
in motivation for food
SB 334867 10 mg/kg
n10
30Orexin/Hcrt 1 receptor signaling is not involved
in motivation for food
SB 334867 20 mg/kg
n12
31Cumulative response shows the pattern of presses
for food in vehicle and SB334867 treated rats
32Cocaine Self-Administration increases OxA/Hcrt1
potentiation of NMDARs
Cocaine
Food
n8
n8
33OxA/Hcrt 1 mediated potentiation of NMDAR is not
different between food restricted (sham) and
naïve rats
Sham
Naive
n7
n9
34Cocaine self-administration potentiates
OxA/Hcrt1-mediated synaptic plasticity in the VTA
35Summary
- OxA/Hcrt1 potentiates NMDA currents in DA neurons
of the VTA. - OxA/Hcrt1 enhance
- synaptic strength in the mesolimbic system
- burst firing of DA neurons, and increase in DA
release. - OxA/Hcrt1 causes a late phase increase in AMPAR
mediated synaptic transmission - Facilitating dopamines role in reinforcement?
36Summary -2
- OXR1/Hcrt1R antagonist blocks cocaine
sensitization, indicating that activation of
orexin/hypocretin 1 receptors in the VTA is
required for the development of sensitization. - Orexin/hypocretin signaling is involved in
motivation for cocaine but not food seeking - Cocaine self-administration potentiates
orexin/hypocretin-mediated plasticity in the VTA
37Acknowledgements
- Sharif Taha
- Federica Sarti
- Shao-Ju Chang
- Billy Chen
Antonello Bonci Howard Fields
- Funding NARSAD
- NIDA (A.B.)
- State of California (A.B.)
38Prolonged application causes a long-lasting
increase in NMDAR EPSCs
n6
39Does OxA/Hcrt1 potentiate NMDARs in dopamine
neurons?
Cameron et al., 1996 Neurosci 77
40OxA/Hcrt1 increases NMDAR EPSCs in VTA
dopaminergic neurons
TH-FITC
Merge
Biocytin-TR
0/2
41Orexin plays a gatekeeper role in that it enables
neuroplasticity in excitatory synapses in the VTA
- Ox/hcrt potentiation of NMDA promotes burst
firing and increases DA release. - Ox/hcrt late phase potentiation of AMPARs may
prolong burst firing. - This plasticity may underlie the intensification
of goal-directed behavior.
Jones Bonci 2005 520-5
42OXR1 antagonist reduces food self-administration
in the presence of cocaine
n12
43OXR1 antagonist reduces breakpoint in the
presence of cocaine
n12
44Dopamine is required for the orexin-mediated
reduction in food seeking
n11
45Dopamine is required for the orexin-mediated
reduction in food seeking
n9
46SB 334867 attenuates potentiation of breakpoint
by a single injection of cocaine
47OXR1 signaling needed for cocaine PR but not food
PR
- Is increased dopamine required for orexin
release? - Can blocking orexin receptors in food treated
rats reduce breakpoint after injection of
GBR12909 (5 mg/kg) or cocaine (15 mg/kg)? -
- Is orexin signaling involved only for highly
motivational substances? - If you increase the reinforcing value of the
reward, ie. Sucrose or high fat, will the orexin
antagonist reduce seeking? - Does cocaine potentiate orexin release/signaling?
48SB 334867 (10 mg/kg) does not reduce motivation
for sucrose
Vehicle SB334867
SB 334867 10 mg/kg
n12
49SB 334867 (20 mg/kg) does not reduce motivation
for sucrose
Vehicle SB334867
SB 334867 20 mg/kg
n9
50OXR1 signaling needed for cocaine PR but not food
PR
- Is increased dopamine required for orexin
release? - Can blocking orexin receptors in food treated
rats reduce breakpoint after injection of
GBR12909 (5 mg/kg) or cocaine (15 mg/kg)? -
- Is orexin signaling involved only for highly
motivational substances? - If you increase the reinforcing value of the
reward, ie. Sucrose or high fat, will the orexin
antagonist reduce seeking? - Does cocaine/dopamine potentiate orexin
release/signaling? - Is there a change in pre-pro orexin in the LH?
- Is there an alteration of orexin-mediated
plasticity in the VTA?
51Future experiments
- Are sucrose pellets not reinforcing enough? Is
orexin signaling involved in motivation for high
fat pellets? - Does chronic cocaine change levels of pre-pro
orexin or orexin A released? - Is the OXR1 antagonist mediating the reduction in
cocaine seeking acting in the VTA?
52Orexin and Self-Administration
- Single injection (icv) of OxA induced persistent
elevations of ICSS thresholds in drug naïve rats
(Boutrel et al., 2006) - OxA (icv) reinstated cocaine food self admin (2
wk extinction) (Boutrel et al., 2006) - OxA induced reinstatement was partially blocked
by adrenergic and CRF antagonists (Boutrel et
al., 2006) - OXR1 antagonist (ip) blocked footshock induced
reinstatement (Boutrel et al., 2006) - OxA (icv) for 3 consecutive days did not alter
cocaine self administration (Boutrel et al., SFN
2004) - OxA (icv) did not alter progressive ratio for
cocaine (0.25 mg/infusion Boutrel et al., SFN
2004)